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狂犬病病毒中一种非致病性糖蛋白基因对致病性糖蛋白基因的显性作用。

Dominance of a nonpathogenic glycoprotein gene over a pathogenic glycoprotein gene in rabies virus.

作者信息

Faber Milosz, Faber Marie-Luise, Li Jianwei, Preuss Mirjam A R, Schnell Matthias J, Dietzschold Bernhard

机构信息

Department of Microbiology and Immunology, Thomas Jefferson University, Philadelphia, PA 19107, USA.

出版信息

J Virol. 2007 Jul;81(13):7041-7. doi: 10.1128/JVI.00357-07. Epub 2007 Apr 25.

Abstract

The nonpathogenic phenotype of the live rabies virus (RV) vaccine SPBNGAN is determined by an Arg-->Glu exchange at position 333 in the glycoprotein, designated GAN. We recently showed that after several passages of SPBNGAN in mice, an Asn-->Lys mutation arose at position 194 of GAN, resulting in GAK, which was associated with a reversion to the pathogenic phenotype. Because an RV vaccine candidate containing two GAN genes (SPBNGAN-GAN) exhibits increased immunogenicity in vivo compared to the single-GAN construct, we tested whether the presence of two GAN genes might also enhance the probability of reversion to pathogenicity. Comparison of SPBNGAN-GAN with RVs constructed to contain either both GAN and GAK genes (SPBNGAN-GAK and SPBNGAK-GAN) or two GAK genes (SPBNGAK-GAK) showed that while SPBNGAK-GAK was pathogenic, SPBNGAN-GAN and SPBNGAN-GAK were completely nonpathogenic and SPBNGAK-GAN showed strongly reduced pathogenicity. Analysis of genomic RV RNA in mouse brain tissue revealed significantly lower virus loads in SPBNGAN-GAK- and SPBNGAK-GAN-infected brains than those detected in SPBNGAK-GAK-infected brains, indicating the dominance of the nonpathogenic phenotype determined by GAN over the GAK-associated pathogenic phenotype. Virus production and viral RNA synthesis were markedly higher in SPBNGAN-, SPBNGAK-GAN-, and SPBNGAN-GAK-infected neuroblastoma cells than in the SPBNGAK- and SPBNGAK-GAK-infected counterparts, suggesting control of GAN dominance at the level of viral RNA synthesis. These data point to the lower risk of reversion to pathogenicity of a recombinant RV carrying two identical GAN genes compared to that of an RV carrying only a single GAN gene.

摘要

狂犬病病毒(RV)活疫苗SPBNGAN的非致病表型由糖蛋白第333位的精氨酸(Arg)替换为谷氨酸(Glu)决定,该糖蛋白被命名为GAN。我们最近发现,SPBNGAN在小鼠体内传代几次后,GAN的第194位出现了天冬酰胺(Asn)替换为赖氨酸(Lys)的突变,产生了GAK,这与致病表型的恢复有关。由于与单GAN构建体相比,含有两个GAN基因的RV候选疫苗(SPBNGAN-GAN)在体内表现出更高的免疫原性,我们测试了两个GAN基因的存在是否也会增加恢复致病力的可能性。将SPBNGAN-GAN与构建为包含GAN和GAK基因(SPBNGAN-GAK和SPBNGAK-GAN)或两个GAK基因(SPBNGAK-GAK)的RV进行比较,结果显示,虽然SPBNGAK-GAK具有致病性,但SPBNGAN-GAN和SPBNGAN-GAK完全无致病性,而SPBNGAK-GAN的致病性则显著降低。对小鼠脑组织中的基因组RV RNA进行分析发现,与SPBNGAK-GAK感染的脑相比,SPBNGAN-GAK和SPBNGAK-GAN感染的脑中病毒载量显著更低,这表明GAN决定的非致病表型对GAK相关的致病表型具有显性作用。在SPBNGAN、SPBNGAK-GAN和SPBNGAN-GAK感染的神经母细胞瘤细胞中,病毒产生和病毒RNA合成明显高于SPBNGAK和SPBNGAK-GAK感染的细胞,这表明在病毒RNA合成水平上存在GAN显性的调控。这些数据表明,与仅携带单个GAN基因的RV相比,携带两个相同GAN基因的重组RV恢复致病力的风险更低。

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